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施马伦贝格病毒包膜蛋白 Gc 的 N 端结构域具有高度免疫原性,可提供针对感染的保护。

The N-terminal domain of Schmallenberg virus envelope protein Gc is highly immunogenic and can provide protection from infection.

机构信息

Institute of Diagnostic Virology, Friedrich-Loeffler-Institut, 17493 Greifswald - Insel Riems, Germany.

出版信息

Sci Rep. 2017 Feb 13;7:42500. doi: 10.1038/srep42500.

Abstract

Schmallenberg virus (SBV) is transmitted by insect vectors, and therefore vaccination is one of the most important tools of disease control. In our study, novel subunit vaccines on the basis of an amino-terminal domain of SBV Gc of 234 amino acids ("Gc Amino") first were tested and selected using a lethal small animal challenge model and then the best performing formulations also were tested in cattle. We could show that neither E. coli expressed nor the reduced form of "Gc Amino" protected from SBV infection. In contrast, both, immunization with "Gc Amino"-encoding DNA plasmids and "Gc-amino" expressed in a mammalian system, conferred protection in up to 66% of the animals. Interestingly, the best performance was achieved with a multivalent antigen containing the covalently linked Gc domains of both, SBV and the related Akabane virus. All vaccinated cattle and mice were fully protected against SBV challenge infection. Furthermore, in the absence of antibodies against the viral N-protein, differentiation between vaccinated and field-infected animals allows an SBV marker vaccination concept. Moreover, the presented vaccine design also could be tested for other members of the Simbu serogroup and might allow the inclusion of additional immunogenic domains.

摘要

舍姆利基森林病毒(SBV)通过昆虫媒介传播,因此疫苗接种是疾病控制的最重要工具之一。在我们的研究中,新型亚单位疫苗是基于 SBV Gc 的氨基末端结构域 234 个氨基酸(“Gc 氨基”),首先使用致死性小动物挑战模型进行了测试和选择,然后对表现最好的配方也在牛中进行了测试。我们发现,无论是大肠杆菌表达的还是还原形式的“Gc 氨基”都不能预防 SBV 感染。相比之下,用“Gc 氨基”编码的 DNA 质粒免疫和在哺乳动物系统中表达的“Gc-amino”都能使高达 66%的动物得到保护。有趣的是,表现最好的是一种含有 SBV 和相关的阿卡斑病毒的共价连接 Gc 结构域的多价抗原。所有接种疫苗的牛和老鼠都完全免受 SBV 挑战感染的侵害。此外,在没有针对病毒 N 蛋白的抗体的情况下,区分接种疫苗和田间感染的动物可以实现 SBV 标记疫苗接种概念。此外,所提出的疫苗设计还可以针对 Simbu 血清群的其他成员进行测试,并可能允许包含其他免疫原性结构域。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/00b5/5304187/6c95379b71eb/srep42500-f1.jpg

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